Taspase1-dependent TFIIA cleavage coordinates head morphogenesis by limiting Cdkn2a locus transcription
Shugaku Takeda, … , Emily H. Cheng, James J. Hsieh
Shugaku Takeda, … , Emily H. Cheng, James J. Hsieh
Published February 9, 2015
Citation Information: J Clin Invest. 2015;125(3):1203-1214. https://doi.org/10.1172/JCI77075.
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Taspase1-dependent TFIIA cleavage coordinates head morphogenesis by limiting Cdkn2a locus transcription

Abstract

Head morphogenesis requires complex signal relays to enable precisely coordinated proliferation, migration, and patterning. Here, we demonstrate that, during mouse head formation, taspase1-mediated (TASP1-mediated) cleavage of the general transcription factor TFIIA ensures proper coordination of rapid cell proliferation and morphogenesis by maintaining limited transcription of the negative cell cycle regulators p16Ink4a and p19Arf from the Cdkn2a locus. In mice, loss of TASP1 function led to catastrophic craniofacial malformations that were associated with inadequate cell proliferation. Compound deficiency of Cdkn2a, especially p16Ink4a deficiency, markedly reduced the craniofacial anomalies of TASP1-deficent mice. Furthermore, evaluation of mice expressing noncleavable TASP1 targets revealed that TFIIA is the principal TASP1 substrate that orchestrates craniofacial morphogenesis. ChIP analyses determined that noncleaved TFIIA accumulates at the p16Ink4a and p19Arf promoters to drive transcription of these negative regulators. In summary, our study elucidates a regulatory circuit comprising proteolysis, transcription, and proliferation that is pivotal for construction of the mammalian head.

Authors

Shugaku Takeda, Satoru Sasagawa, Toshinao Oyama, Adam C. Searleman, Todd D. Westergard, Emily H. Cheng, James J. Hsieh

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Figure 5

Genetic knockin of cleavage-resistant forms of TASP1 substrates reveals that noncleavage of TFIIAα-β phenocopies the craniofacial malformations observed in Tasp1–/– mice.

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Genetic knockin of cleavage-resistant forms of TASP1 substrates reveals ...
(A) Mll1nc/nc, Mll2nc/nc, and Mll1nc/nc Mll2nc/nc mice at P0 did not display craniofacial defects. Scale bar: 2.0 mm. (B) WT, Tfiia+/nc, and Tfiianc/nc mice obtained from Tfiia+/nc intercrosses were observed at the expected Mendelian ratios at the indicated developmental stages. Nearly 100% of Tfiianc/nc mice died within the first day of birth. (C) Tfiianc/nc P0 animals exhibited head malformations similar to those observed in Tasp1–/– animals. Scale bar: 2.0 mm. (D) WT and Tfiianc/nc E10.5 and E14.5 embryos with head malformations. Frequencies of the otocephalic phenotypes in E14.5 WT, Tfiia+/nc, and Tfiianc/nc embryos are shown. Scale bar: 1.0 mm.